Cancer therapies activate RIG-I-like receptor pathway through endogenous non-coding RNAs

Emerging evidence indicates that ionizing radiation (IR) and chemotherapy activate Type I interferon (IFN) signaling in tumor and host cells. However, the mechanism of induction is poorly understood. We identified a novel radioprotective role for the DEXH box RNA helicase LGP2 (DHX58) through its su...

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Autores principales: Ranoa, Diana Rose E., Parekh, Akash D., Pitroda, Sean P., Huang, Xiaona, Darga, Thomas, Wong, Anthony C., Huang, Lei, Andrade, Jorge, Staley, Jonathan P., Satoh, Takashi, Akira, Shizuo, Weichselbaum, Ralph R., Khodarev, Nikolai N.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5041995/
https://www.ncbi.nlm.nih.gov/pubmed/27034163
http://dx.doi.org/10.18632/oncotarget.8420
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author Ranoa, Diana Rose E.
Parekh, Akash D.
Pitroda, Sean P.
Huang, Xiaona
Darga, Thomas
Wong, Anthony C.
Huang, Lei
Andrade, Jorge
Staley, Jonathan P.
Satoh, Takashi
Akira, Shizuo
Weichselbaum, Ralph R.
Khodarev, Nikolai N.
author_facet Ranoa, Diana Rose E.
Parekh, Akash D.
Pitroda, Sean P.
Huang, Xiaona
Darga, Thomas
Wong, Anthony C.
Huang, Lei
Andrade, Jorge
Staley, Jonathan P.
Satoh, Takashi
Akira, Shizuo
Weichselbaum, Ralph R.
Khodarev, Nikolai N.
author_sort Ranoa, Diana Rose E.
collection PubMed
description Emerging evidence indicates that ionizing radiation (IR) and chemotherapy activate Type I interferon (IFN) signaling in tumor and host cells. However, the mechanism of induction is poorly understood. We identified a novel radioprotective role for the DEXH box RNA helicase LGP2 (DHX58) through its suppression of IR-induced cytotoxic IFN-beta [1]. LGP2 inhibits activation of the RIG-I-like receptor (RLR) pathway upon binding of viral RNA to the cytoplasmic sensors RIG-I (DDX58) and MDA5 (IFIH1) and subsequent IFN signaling via the mitochondrial adaptor protein MAVS (IPS1). Here we show that MAVS is necessary for IFN-beta induction and interferon-stimulated gene expression in the response to IR. Suppression of MAVS conferred radioresistance in normal and cancer cells. Germline deletion of RIG-I, but not MDA5, protected mice from death following total body irradiation, while deletion of LGP2 accelerated the death of irradiated animals. In human tumors depletion of RIG-I conferred resistance to IR and different classes of chemotherapy drugs. Mechanistically, IR stimulated the binding of cytoplasmic RIG-I with small endogenous non-coding RNAs (sncRNAs), which triggered IFN-beta activity. We demonstrate that the small nuclear RNAs U1 and U2 translocate to the cytoplasm after IR treatment, thus stimulating the formation of RIG-I: RNA complexes and initiating downstream signaling events. Taken together, these findings suggest that the physiologic responses to radio-/chemo-therapy converge on an antiviral program in recruitment of the RLR pathway by a sncRNA-dependent activation of RIG-I which commences cytotoxic IFN signaling. Importantly, activation of interferon genes by radiation or chemotherapy is associated with a favorable outcome in patients undergoing treatment for cancer. To our knowledge, this is the first demonstration of a cell-intrinsic response to clinically relevant genotoxic treatments mediated by an RNA-dependent mechanism.
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spelling pubmed-50419952016-10-10 Cancer therapies activate RIG-I-like receptor pathway through endogenous non-coding RNAs Ranoa, Diana Rose E. Parekh, Akash D. Pitroda, Sean P. Huang, Xiaona Darga, Thomas Wong, Anthony C. Huang, Lei Andrade, Jorge Staley, Jonathan P. Satoh, Takashi Akira, Shizuo Weichselbaum, Ralph R. Khodarev, Nikolai N. Oncotarget Research Paper Emerging evidence indicates that ionizing radiation (IR) and chemotherapy activate Type I interferon (IFN) signaling in tumor and host cells. However, the mechanism of induction is poorly understood. We identified a novel radioprotective role for the DEXH box RNA helicase LGP2 (DHX58) through its suppression of IR-induced cytotoxic IFN-beta [1]. LGP2 inhibits activation of the RIG-I-like receptor (RLR) pathway upon binding of viral RNA to the cytoplasmic sensors RIG-I (DDX58) and MDA5 (IFIH1) and subsequent IFN signaling via the mitochondrial adaptor protein MAVS (IPS1). Here we show that MAVS is necessary for IFN-beta induction and interferon-stimulated gene expression in the response to IR. Suppression of MAVS conferred radioresistance in normal and cancer cells. Germline deletion of RIG-I, but not MDA5, protected mice from death following total body irradiation, while deletion of LGP2 accelerated the death of irradiated animals. In human tumors depletion of RIG-I conferred resistance to IR and different classes of chemotherapy drugs. Mechanistically, IR stimulated the binding of cytoplasmic RIG-I with small endogenous non-coding RNAs (sncRNAs), which triggered IFN-beta activity. We demonstrate that the small nuclear RNAs U1 and U2 translocate to the cytoplasm after IR treatment, thus stimulating the formation of RIG-I: RNA complexes and initiating downstream signaling events. Taken together, these findings suggest that the physiologic responses to radio-/chemo-therapy converge on an antiviral program in recruitment of the RLR pathway by a sncRNA-dependent activation of RIG-I which commences cytotoxic IFN signaling. Importantly, activation of interferon genes by radiation or chemotherapy is associated with a favorable outcome in patients undergoing treatment for cancer. To our knowledge, this is the first demonstration of a cell-intrinsic response to clinically relevant genotoxic treatments mediated by an RNA-dependent mechanism. Impact Journals LLC 2016-03-28 /pmc/articles/PMC5041995/ /pubmed/27034163 http://dx.doi.org/10.18632/oncotarget.8420 Text en Copyright: © 2016 Ranoa et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Ranoa, Diana Rose E.
Parekh, Akash D.
Pitroda, Sean P.
Huang, Xiaona
Darga, Thomas
Wong, Anthony C.
Huang, Lei
Andrade, Jorge
Staley, Jonathan P.
Satoh, Takashi
Akira, Shizuo
Weichselbaum, Ralph R.
Khodarev, Nikolai N.
Cancer therapies activate RIG-I-like receptor pathway through endogenous non-coding RNAs
title Cancer therapies activate RIG-I-like receptor pathway through endogenous non-coding RNAs
title_full Cancer therapies activate RIG-I-like receptor pathway through endogenous non-coding RNAs
title_fullStr Cancer therapies activate RIG-I-like receptor pathway through endogenous non-coding RNAs
title_full_unstemmed Cancer therapies activate RIG-I-like receptor pathway through endogenous non-coding RNAs
title_short Cancer therapies activate RIG-I-like receptor pathway through endogenous non-coding RNAs
title_sort cancer therapies activate rig-i-like receptor pathway through endogenous non-coding rnas
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5041995/
https://www.ncbi.nlm.nih.gov/pubmed/27034163
http://dx.doi.org/10.18632/oncotarget.8420
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